ACUTE BEHAVIORAL TOXICITY OF PYRIDOSTIGMINE OR SOMAN IN PRIMATES

被引:23
作者
BLICK, DW
MURPHY, MR
BROWN, GC
YOCHMOWITZ, MG
FANTON, JW
HARTGRAVES, SL
机构
[1] USAF,ARMSTRONG LAB,DIV DIRECTED ENERGY,BROOKS AFB,TX 78235
[2] USAF,ARMSTRONG LAB,DIV VET SCI,BROOKS AFB,TX 78235
关键词
D O I
10.1006/taap.1994.1121
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Effects of a peripherally active carbamate (pyridostigmine bromide) and a centrally active organophosphate (OP) nerve agent (soman) on performance by rhesus monkeys of a compensatory tracking (primate equilibrium platform, or PEP) task were measured using a balanced Latin-square design to determine the ED50 for pyridostigmine (0.66 mg/kg) and the up-and-down (titration) method to determine the ED50 for soman (2.50 mu g/kg). We concluded that the PEP performance model is a sensitive and reliable indicator of anticholinesterase (anti-ChE) behavioral toxicity. We also found that soman, an irreversible inhibitor of acetylcholinesterase (AChE), is more than 100 times more behaviorally disruptive than the reversible peripheral inhibitor pyridostigmine, as indicated by the difference in ED50 doses expressed in molar terms. Soman's behavioral toxicity is severe at levels of serum cholinesterase inhibition (70-80%) at which pyridostigmine does not significantly affect performance. As a prophylactic treatment for OP agent poisoning, pyridostigmine has a substantial safety factor, since behavioral toxicity becomes significant only at approximately four times the proposed therapeutic dose. (C) 1994 Academic Press, Inc.
引用
收藏
页码:311 / 318
页数:8
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